Asymmetric Tandem Additions to Chiral 2,3-Dihydronaphthyloxazolines: Synthesis of the Triptoquinone/Triptinin A Ring System

 

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Abstract

A study to reach the diterpenoid (+)-triptoquinone A (3) or its analog (+)-triptinin A (4) via an asymmetric tandem addition to naphthyloxazolines is described. The tandem addition to the chiral dihydronophthalene 6 resulted in a 70% yield of a single diastereomer 10. Further manipulation gave the natural products’ tricyclic ring system, compounds 20 and 29 via ring-closing metathesis in 90% yield, using the Schrock catalyst. Final assault to the target compounds 3 or 4 fell short due to the failure to either reduce a neopentyl hydroxymethyl group to a methyl or to install the conjugated carboxylic acid present in 3 or 4.

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Compound 12 was prepared as described in the experimental.

Attempts were made to use a vinyl bromide into the tandem product below. However, the electrophilic step in the tandem addition failed. Presumably, the azaenolate, formed upon the addition of the 2-lithiopropene, is too basic and causes elimination of HBr from 1,3-dibromobut-3-ene (Scheme [] 11).

The yield of this reaction was dependent upon the quality of the catalyst (purchased from Strem Chemical Company) as evidenced by its often dark color.

300 MHz ¹H NMR spectra of 32-34 and 38 are included in the supplementary material.